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Reference Report

Reference
Citation	Makki, R., Meister, M., Pennetier, D., Ubeda, J.M., Braun, A., Daburon, V., Krzemień, J., Bourbon, H.M., Zhou, R., Vincent, A., Crozatier, M. (2010). A short receptor downregulates Jak/STAT signalling to control the Drosophila cellular immune response.  PLoS Biol. 8(8): e1000441. (Export to RIS)
FlyBase ID	FBrf0211466
Publication Type	Research paper
PubMed ID	20689801
PubMed Abstract	The posterior signalling centre (PSC), a small group of specialised cells, controls hemocyte (blood cell) homeostasis in the Drosophila larval hematopoietic organ, the lymph gland. This role of the PSC is very reminiscent of the "niche," the micro-environment of hematopoietic stem cells in vertebrates. We have recently shown that the PSC acts in a non-cell-autonomous manner to maintain janus tyrosine kinase/signal transducers and activators of transcription (JAK/STAT) signalling in hematopoietic progenitors (prohemocytes), thereby preserving the multipotent character necessary for their differentiation into lamellocytes, a cryptic and dedicated immune cell type required to fight specific immune threats such as wasp parasitism. In this report, on the basis of a knock out generated by homologous recombination, we show that a short type I cytokine-related receptor CG14225/Latran is required for switching off JAK/STAT signalling in prohemocytes. This is a prerequisite to massive differentiation of lamellocytes upon wasp parasitisation. In vivo and cell culture assays indicate that Latran forms heteromers with Domeless, the Drosophila type I cytokine signalling receptor related to mammalian GP130, and antagonises Domeless activity in a dose-dependent manner. Our analysis further shows that a primary immune response to wasp parasitism is a strong decrease in cytokine mRNA levels in the lymph gland, followed by an increase in the latran/domeless ratio. We propose that this sequence of events culminates in the complete inhibition of residual JAK/STAT signalling by Latran. JAK/STAT activity has been associated with several human diseases including leukaemia while knock-out studies in mice point to a central role of this pathway in hematopoiesis and regulation of immune functions. The specific function of Drosophila Latran is, to our knowledge, the first in vivo example of a role for a nonsignalling receptor in controlling a dedicated immune response, and thus raises the question of whether short, nonsignalling receptors also control specific aspects of vertebrate cellular immunity.
DOI	10.1371/journal.pbio.1000441
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Description	What does this section display? This section contains items that were added to this record for each release. It currently only tracks new links between this FlyBase report and other FlyBase data classes (e.g. genes, references, stocks) or controlled vocabulary terms (e.g. GO, anatomy terms). What does this section not display? This section does not currently display links that were removed or gene model changes.
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Associated Information
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Secondary IDs
Language of Publication	English
Additional Languages of Abstract
Also Published As
Parent Publication
Publication Type	Journal
Abbreviation	PLoS Biol.
Title	PLoS Biology
Publication Year	2003-
ISBN/ISSN	1545-7885 1544-9173
Data from Reference
Alleles (18)
	domePG125 domeScer\UAS.cCGHa domeScer\UAS.T:Ecol\lacZ-Δα domeScer\UAS.T:Ecol\lacZ-Δω Ecol\lacZMESO.dome.hs et18A etScer\UAS.cMa etScer\UAS.T:Ecol\lacZ-Δα etScer\UAS.T:Ecol\lacZ-Δω hopdsRNA.Scer\UAS.cMa Mmus\Cd8aScer\UAS.T:Avic\GFP Scer\GAL4da.G32 Scer\GAL4dome-PG125 Scer\GAL4ey.PH Scer\GAL4kn-col85-GAL4 Scer\GAL4srp.D.cCa Stat92EScer\UAS.T:Avic\GFP-EGFP upd3dsRNA.Scer\UAS
Constructs (14)
	P{dome-lacZ.MESO} P{GAL4-da.G32} P{GAL4-ey.H} P{srpD-GAL4.C} P{UAS-dome.CGH} P{UAS-dome.Δα} P{UAS-dome.Δω} P{UAS-et.M} P{UAS-et.Δα} P{UAS-et.Δω} P{UAS-hop.dsRNA.M} P{UAS-mCD8::GFP.L} P{UAS-Stat92E.EGFP} P{UAS-upd3.dsRNA}
Genes (12)
	crl dome Ecol\lacZ et hop ItgαPS4 Mmus\Cd8a Scer\GAL4 Stat92E T:Ecol\lacZ Tep4 upd3
Insertions (2)
	P{GAL4}col85 P{GawB}domePG125
Natural transposons (1)
	P-element